Single xenotransplant of rat brown adipose tissue prolonged the ovarian lifespan of aging mice by improving follicle survival

生物 异种移植 卵巢 同种异体移植 毛囊 转录组 脂肪组织 DNA甲基化 男科 内科学 内分泌学 移植 基因 遗传学 基因表达 医学
作者
Liang‐Jian Chen,Zhi‐Xia Yang,Yang Wang,Lei Du,Yan‐Ru Li,Nana Zhang,Wen‐Yi Gao,Rui‐Rui Peng,Fengyu Zhu,Lili Wang,Cong‐Rong Li,Jianmin Li,Fuqiang Wang,Qing‐Yuan Sun,Dong Zhang
出处
期刊:Aging Cell [Wiley]
卷期号:18 (6) 被引量:25
标识
DOI:10.1111/acel.13024
摘要

Abstract Prolonging the ovarian lifespan is attractive and challenging. An optimal clinical strategy must be safe, long‐acting, simple, and economical. Allotransplantation of brown adipose tissue (BAT), which is most abundant and robust in infants, has been utilized to treat various mouse models of human disease. Could we use BAT to prolong the ovarian lifespan of aging mice? Could we try BAT xenotransplantation to alleviate the clinical need for allogeneic BAT due to the lack of voluntary infant donors? In the current study, we found that a single rat‐to‐mouse (RTM) BAT xenotransplantation did not cause systemic immune rejection but did significantly increase the fertility of mice and was effective for more than 5 months (equivalent to 10 years in humans). Next, we did a series of analysis including follicle counting; AMH level; estrous cycle; mTOR activity; GDF9, BMP15, LHR, Sirt1, and Cyp19a level; ROS and annexin V level; IL6 and adiponectin level; biochemical blood indices; body temperature; transcriptome; and DNA methylation studies. From these, we proposed that rat BAT xenotransplantation rescued multiple indices indicative of follicle and oocyte quality; rat BAT also improved the metabolism and general health of the aging mice; and transcriptional and epigenetic (DNA methylation) improvement in F0 mice could benefit F1 mice; and multiple KEGG pathways and GO classified biological processes the differentially expressed genes (DEGs) or differentially methylated regions (DMRs) involved were identical between F0 and F1. This study could be a helpful reference for clinical BAT xenotransplantation from close human relatives to the woman.

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